Nanoparticle-mediated Photodynamic Therapy as a Method to Ablate Oral Cavity Squamous Cell Carcinoma in Preclinical Models

Author:

Sahovaler Axel123ORCID,Valic Michael S.34ORCID,Townson Jason L.23ORCID,Chan Harley H.L.23ORCID,Zheng Mark3ORCID,Tzelnick Sharon123ORCID,Mondello Tiziana123ORCID,Pener-Tessler Alon123ORCID,Eu Donovan123ORCID,El-Sayes Abdullah3ORCID,Ding Lili3ORCID,Chen Juan3ORCID,Douglas Catriona M.125ORCID,Weersink Robert236ORCID,Muhanna Nidal127ORCID,Zheng Gang346ORCID,Irish Jonathan C.123ORCID

Affiliation:

1. 1Department of Otolaryngology–Head and Neck Surgery, University of Toronto, Toronto, Ontario, Canada.

2. 2TECHNA Institute, Guided Therapeutics (GTx) Program, University Health Network, Toronto, Ontario, Canada.

3. 3Princess Margaret Cancer Centre, University Health Network, Toronto, Ontario, Canada.

4. 4Institute of Biomedical Engineering (BME), University of Toronto, Toronto, Ontario, Canada.

5. 5Department of Otolaryngology–Head and Neck Surgery, Queen Elizabeth University Hospital, Glasgow, United Kingdom.

6. 6Department of Medical Biophysics, University of Toronto, Toronto, Ontario, Canada.

7. 7Department of Otolaryngology–Head and Neck Surgery, Tel Aviv Sourasky Medical Centre, Tel Aviv University, Tel Aviv, Israel.

Abstract

Abstract Photodynamic therapy (PDT) is a tissue ablation technique able to selectively target tumor cells by activating the cytotoxicity of photosensitizer dyes with light. PDT is nonsurgical and tissue sparing, two advantages for treatments in anatomically complex disease sites such as the oral cavity. We have previously developed PORPHYSOME (PS) nanoparticles assembled from chlorin photosensitizer–containing building blocks (∼94,000 photosensitizers per particle) and capable of potent PDT. In this study, we demonstrate the selective uptake and curative tumor ablation of PS-enabled PDT in three preclinical models of oral cavity squamous cell carcinoma (OCSCC): biologically relevant subcutaneous Cal-33 (cell line) and MOC22 (syngeneic) mouse models, and an anatomically relevant orthotopic VX-2 rabbit model. Tumors selectively uptake PS (10 mg/kg, i.v.) with 6-to 40-fold greater concentration versus muscle 24 hours post-injection. Single PS nanoparticle–mediated PDT (PS-PDT) treatment (100 J/cm2, 100 mW/cm2) of Cal-33 tumors yielded significant apoptosis in 65.7% of tumor cells. Survival studies following PS-PDT treatments demonstrated 90% (36/40) overall response rate across all three tumor models. Complete tumor response was achieved in 65% of Cal-33 and 91% of MOC22 tumor mouse models 14 days after PS-PDT, and partial responses obtained in 25% and 9% of Cal-33 and MOC22 tumors, respectively. In buccal VX-2 rabbit tumors, combined surface and interstitial PS-PDT (200 J total) yielded complete responses in only 60% of rabbits 6 weeks after a single treatment whereas three repeated weekly treatments with PS-PDT (200 J/week) achieved complete ablation in 100% of tumors. PS-PDT treatments were well tolerated by animals with no treatment-associated toxicities and excellent cosmetic outcomes. Significance: PS-PDT is a safe and repeatable treatment modality for OCSCC ablation. PS demonstrated tumor selective uptake and PS-PDT treatments achieved reproducible efficacy and effectiveness in multiple tumor models superior to other clinically tested photosensitizer drugs. Cosmetic and functional outcomes were excellent, and no clinically significant treatment-associated toxicities were detected. These results are enabling of window of opportunity trials for fluorescence-guided PS-PDT in patients with early-stage OCSCC scheduled for surgery.

Funder

Terry Fox Research Institute

Princess Margaret Cancer Foundation

Publisher

American Association for Cancer Research (AACR)

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